Furthermore, the echogenicity of contralateral thalamus, contralateral lenticular nucleus and contralateral
caudate nucleus should be evaluated semiquantitatively. Normally, these structures are invisible, i.e., isoechogenic to the surrounding brain parenchyma. Sometimes, the borders of the ipsilateral internal capsule can be detected, allowing a separation of the thalamus from the lenticular nucleus. An increased echogenicity (‘hyperechogenicity’) of thalamus, lenticular nucleus or caudate nucleus compared with surrounding white matter is considered to be abnormal. Hyperechogenicity of deep brain AUY-922 in vitro structures is often caused by trace metal accumulation or by calcification [2]. In the latter case, the echosignals are very bright, similar to that of pineal gland [30]. Two of the earliest published TCS applications in adults were the detection of intracranial hematomas in acute stroke or trauma patients [8], [10] and [31], and the assessment of the ventricular system [11]. While computed tomography (CT) and MRI today represent the gold standard in the diagnosis of intracranial hemorrhage [32] and [33], TCS can well be used for the bedside monitoring for the size
and resorption of hematomas, and, especially for the monitoring of midline shift. In the acute phase, intracerebral hemorrhage (ICH) appears homogenous, sharply demarcated and hyperechogenic (Fig. 4) [31]. In 1993, Seidel et al. [8] were the first to describe an alteration of the sonographic Tenofovir price appearance of ICH over time with a decrease in echo intensity beginning at the center of the lesion. They were able
to detect the ICH with ultrasound in 18 of 23 patients (78%). Insufficient insonation conditions were found in 13% of patients. In a prospective TCS study of 151 patients with acute hemiparesis of whom 60 had an ICH on CT, TCS differentiated correctly between ischemia and hemorrhage in 95% of the assessable patients [34]. Insufficient insonation conditions were found in 12% of patients. In a more recent study of 25 patients with confirmed subdural hematoma, TCS detected the hematoma in 22 (88%) patients while the temporal bone window was insufficient in 3 (12%) patients [35]. Large hemorrhagic transformations of ischemic infarctions have also been reliably detected with TCS [36] and [37]. A recent study found a good agreement between TCS and CT measures of hematoma volumes [38]. The first www.selleck.co.jp/products/Decitabine.html TCS studies that specifically addressed the value of TCS in the evaluation of midline shift in patients with space-occupying brain infarctions were published by the group of Kaps and co-workers [39], [40] and [41]. In these studies a high correlation between TCS and CT measures of midline shift at the level of third ventricle was found. All patients with an MLS < 4 mm at 32 h survived, whereas patients with an MLS > 4 mm died, as a result of cerebral herniation with an exception of one patient who underwent decompressive hemicraniectomy [40] and [41].